CLL and Lymphoproliferative Disorders

Question 1

Reed Sternberg Cells

Answer 1

Classical Hodgkin Lymphoma

Question 2

NHL

Answer 2

Neoplastic proliferation of lymphoid cells.
Originates in lymphoid tissue (lymph nodes, bone marrow, spleen)
Incidence rising 200/million population/year

Fastest growing human cancer (Burkitt Lymphoma)
Indolent diseases with a 25 year survival

Question 3

Presentation of NHL

Answer 3

Painless lymphadenopathy
Compression symptoms
B symptoms

Question 4

Why is a biopsy taken in NHL

Answer 4

WHO classification of lymphoma subtype

Question 5

Management NHL

Answer 5

Stage the disease: CT scan, PET scan (indicated in aggressive lymphomas), BM biopsy, LP (if risk of CNS involvement)
Prognostic markers and important tests: LDH, performance status, HIV serology (if appropriate HTLV1 serology), Hepatitis B serology (risk of reactivation if B cell depleting therapy given)
Plan therapy: urgent chemotherapy, monitor only, antibiotic eradication (H.pylori gastric MALT lymphoma)

Question 6

NHL subtypes

Answer 6

Follicular lymphoma 
Small lymphocyte lymphoma 
Marginal zone lymphoma 
Diffuse large B cell lymphoma 
Burkitt's lymphoma
B cell lymphoblastic lymphoma 
Mantle cell lymphoma 
Lymphoblastic lymphoma 
NK cell/T cell lymphoma

Question 7

Very aggressive NHL

Answer 7

Burkitt lymphoma

T or B cell lymphoblastic leukaemia/lymphoma

Question 8

Aggressive NHL

Answer 8

Diffuse large B cell

Mantle cell

Question 9

Indolent NHL

Answer 9

Follicular
Small lymphocytic/CLL
Mucosa associated (MALT)

Question 10

Incurable NHL

Answer 10

Indolent forms

Prognosis 10-15 years

Question 11

Curable NHL

Answer 11

Very aggressive forms

Prognosis 2-5 weeks (without treatment)

Question 12

How are very aggressive NHL treated

Answer 12

The same as for acute leukaemia

Question 13

Features of DLBCL

Answer 13

Aggressive B cell NHL
30-40% of all NHL

Prognosis and treatment determined by:
Precise histological diagnosis
Anatomical stage
IPI (International Prognostic Index)

Question 14

What is the IPI for DLBCL

Answer 14

Age > 60y
serum LDH > normal
performance status 2-4
stage III or IV
more than one extranodal site

5 year predicted survival is by number of risk factors: 
0-1 = 73%
2 = 51%
3 = 43%
4-5 = 26%

Question 15

Treatment of DLBCL

Answer 15

Treated by x 6-8 cycles of R-CHOP (Rituximab-CHOP)

combination chemotherapy using a mixture of drugs usually including an anthracycline (e.g. doxorubicin).

Combination drug regimens e.g. CHOP
Cyclophosphamide 750mg/m2 IV
Adriamycin 50mg/m2 IV
Vincristine 1.4mg/m2 IV
Prednisolone 40mg/m2 PO

R is Immunotherapy using the anti CD20 monoclonal antibody Rituximab

Aim of therapy is curative (overall approx 50%)

Relapse: Autologous Stem Cell transplant salvage 25% of patients

Question 16

Features of follicular NHL

Answer 16

Indolent lymphoma
35% of NHL
Associated with t(14;18) which results in over-expression of bcl2 an anti-apoptosis protein
FLIPI score (modified IPI)
Incurable, median survival 12-15 years
May require 2-3 different chemotherapy schedules over the 12-15 year period

Question 17

Treatment of follicular NHL

Answer 17

Indolent slow progressing B cell NHL
Incurable
variable/long natural history

At presentation Watch and wait only treat “if clinically indicated”
Nodes compressing;eg bowel, ureter, vena cava
Massive painful nodes, recurrent infections

Treatment:
combination Immuno-chemotherapy R-CVP
Maintenance rituximab delays Time to next progression
Conventional treatment is not curative

Question 18

Features of MALT lymphomas

Answer 18

Is a Marginal zone NHL involving extranodal lymphoid tissue (ie mucosa-associated lymphoid tissue MALT)
Comprise ~ 8% of all NHL
Chronic antigen stimulation
Sjogrens syndrome ; parotid lymphoma (MZL)
H.Pylori ; Gastric MALT lymphoma (MZL)
Hashimoto’s Thyroid; Thyroid (MZL)
Lachrymal gland (?Psittaci infection)
Median age at presentation 55-60y
Most commonly arise in stomach, usually present with dyspepsia or epigastric pain
Usual presentation is Stage I[E]
‘B’-symptoms uncommon

Question 19

Pathogenesis of MALT lymphomas

Answer 19

Proliferation polyclonal antigen specific B cells (due to chronic gastritis caused by h.pylori infection)
Antigen dependent transformed B cell clone (at this point is an antibiotic sensitive MALT)
Antigen independent transformed B cells (antibiotic insensitive MALT)

Question 20

Treatment of gastric MALT (MZL) stage 1-2 disease

Answer 20

Omep 20mg/Clarith 500mg/amox 1gm bd
Repeat breath test at 2 months
Repeat endoscopy every 6 months for 1st 2years then annually

Durable remission in 75% of patients
response may be delayed until 1yr
If fails eradication therapy then may require chemotherapy

Question 21

Features of CLL

Answer 21

Proliferation of mature B-lymphocytes 
Commonest leukaemia in the western world
Caucasian 
UK incidence 4.2/100,000/year
Age at presentation median 72  (10% aged  <55yrs)
Relatives x7 increased incidence

Question 22

Laboratory findings in CLL

Answer 22

Lymphocytosis between 5 and 300 x 109/l 
Smear cells
Normocytic normochromic anaemia
Thrombocytopenia
Bone marrow	Lymphocytic replacement of normal marrow elements

Question 23

Important targets in CLL treatment

Answer 23

sIg
CD19
CD5

Question 24

Diagnostic algorithm in CLL

Answer 24

Lymphocytes + morphology –> immature lymphoblastic (TdT positive) think acute lymphoblastic leukaemia (ALL)

Lymphocytes + morphology –> small mature lymphocytes + smear cells (need immunopheotype) –> mature B cells CD5 +ve (COULD BE A MANTLE CELL LYMPHOMA) –> immunophenotype CLL score 4-5/5 –> CLL

Question 25

What is the CLL score

Answer 25

CD5
CD23
FMC7
CD79b
SmIg

Question 26

Prognostic factors in CLL

Answer 26

Clinical (quantify the burden of malignant cells) :
Rai staging
Binet staging

Laboratory/malignant cell based:
CD38 expression bad prognosis
Cytogenetics (FISH panel)
Immunglobulin gene mutation status: IgH mutated, IgH unmutated

Question 27

How is clinical stage determined in CLL

Answer 27

Stage A: <3 lymphoid areas
B: >3 lymphoid areas
C: >3 lymphoid areas, Hb<100, platelets <100

Question 28

What are the steps of normal B cell development

Answer 28

Stem cells produce primary repertoire, undergo VDJ joining to produce low affinity antigen specific B cells, which then undergo class switching to produce high affinity antigen-specific B cells

Class switching can lead to IgH mutations. Unmutated VH accounts for 56% of CLL, whilst mutated VH accounts for 44% of CLL.

Question 29

What IgH is associated with better long-term prognosis in CLL

Answer 29

Mutated median survival 25 years

Unmutated median survival is 8 years

Question 30

What chromosomal abnormality is associated with a worse prognosis in CLL

Answer 30

Deletion of 17p - median survival is 32 months

Question 31

Malignant (non functional) mature B cells+ hypogammaglobulinaemia

Clinical issue?

Answer 31

Increased risk of infection

Question 32

Proliferate within Bone marrow (efface)

Clinical issue?

Answer 32

Bone marrow failure

Question 33

Circulating to nodes, spleen and blood

Clinical issue?

Answer 33

Lymphadenopathy +/- splenomegaly, lymphocytosis

Question 34

Acquired further mutations

Clinical issue?

Answer 34

Transform to high grade lymphoma

Question 35

Disease of immune cells

Clinical issue?

Answer 35

Auto-immune complications e.g. haemolytic anaemia

Question 36

Treatment principles in CLL

Answer 36

Suportive treatment:
Vaccination
Anti-infective prophylaxis and treatment

Specific scenarios:
Auto-immune cytopaenias
High grade (Richter) transformation

Leukaemia directed treatment: Tailored to patient

Question 37

Principles of supportive treatment in CLL

Answer 37

Prophylaxis and treatment of infections:
Account for 50% of all CLL related deaths
Most are bacterial, but fungal and viral are becoming increasingly prevalent
Prophylaxis: Aciclovir, PCP prophylaxis for those receiving fludarabine or alemtuzumab (Campath)
IVIG is recommended for those with hypogammaglobulinemia and recurrent bacterial infections, Immunisation against pneumococcus, and seasonal flu

Question 38

Management of auto-immune phenomena in CLL

Answer 38

Auto-immune phenomena:
1st Line Steroids
2nd Line Rituximab

Irradiated Blood products if risk of TA GVHD

Question 39

Richter’s syndrome

Answer 39

CLL transformation to high grade lymphoma

Question 40

Principles of leukaemia directed treatment in CLL

Answer 40

Incurable by chemotherapy: Watch and wait versus active treatment

Conventional not to treat Stage A: What are the indications for treatment?

If required tailor treatment (age/co-morbidities)

Aim of therapy obtain response/remission: disease will relapse, 2nd line therapy

Young patients may be cured by allogeneic stem cell transplants

Question 41

Indications for CLL treatment

Answer 41

Watch and wait unless:
Progressive lymphocytosis
lymphocyte doubling time <6 months
Progressive marrow failure 
Hb < 100, platelets <100, neutrophils <1
Massive or progressive lymphadenopathy/splenomegaly
Systemic symptoms  (B symptoms)
Autoimmune cytopenias  (treat with steroids)

Question 42

Chemo-immunotherapy for CLL

Answer 42

1st line 
Given if TP53 intact 
FCR: fludarabine cyclophosphamide, rituximab (anti CD20)
Rituximab-Bendamustine 
Obinutuzumab (anti CD20) + chlorambucil 
Supportive care only

Question 43

How are high risk CLL cases managed

Answer 43

Patients with TP53/17p deleted CLL 1st Line
Refractory disease or early relapse (<24 months)
Patients failed 2 lines of chemotherapy
New agents: ibrutinib (bruton tyrosine kinase inhibitor), venetoclax 9anti Bcl2 oral agent)

Question 44

Emerging treatment options for CLL

Answer 44

BCR kinase inhibitors: ibrutinib, idelalisib
BCL2 inhibitors: venetoclax
Experimental cell based therapies: chimaeric antigen receptor T cells (CAR-T)